Role of protein kinase C-{varepsilon} (PKC{varepsilon}) in isoflurane-induced cardioprotection

doi:10.1093/bja/aei022

BJA Advance Access originally published online on November 12, 2004
British Journal of Anaesthesia 2005 94(2):166-173; doi:10.1093/bja/aei022

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Role of protein kinase C- ${varepsilon}$ (PKC ${varepsilon}$ ) in isoflurane-induced cardioprotection

D. Obal, N. C. Weber, K. Zacharowski, O. Toma, S. Dettwiler, J. I. Wolter, M. Kratz, J. Müllenheim, B. Preckel and W. Schlack^*

Department of Anesthesiology, University Hospital, Moorenstraße 5, 40225 Düsseldorf, Germany

^* Corresponding author. E-mail: schlack{at}uni-duesseldorf.de

Background. Volatile anaesthetics precondition the heart againstinfarction, an effect partly mediated by activation of the ${varepsilon}$ isoform of protein kinase C (PKC ${varepsilon}$ ). We investigated whether cardioprotectionby activation of PKC ${varepsilon}$ depends on the isoflurane concentration.

Methods. Anaesthetized rats underwent 25 min of coronary arteryocclusion followed by 120 min of reperfusion and were randomlyassigned to the following groups (n=10 in each group): isofluranepreconditioning induced by 15 min administration of 0.4 minimalalveolar concentration (MAC) (0.4MAC), 1 MAC (1MAC) or 1.75MAC (1.75MAC) followed by 10 min washout before ischaemia. Eachprotocol was repeated in the presence of the PKC inhibitor staurosporine(10 µg kg^–1): 0.4MAC+S, 1MAC+S and 1.75MAC+S. Controlswere untreated (CON) and additional hearts received staurosporinewithout isoflurane (S). In a second set of experiments (n=6in each group) hearts were excised before the infarct inducingischaemia, and phosphorylation and translocation of PKC ${varepsilon}$ weredetermined by western blot analysis.

Results. Isoflurane reduced infarct size from a mean of 61(SEM2)% of the area at risk in controls to 20(1)% (0.4MAC), 26(3)%(1MAC) and 30(1)% (1.75MAC) (all P<0.01 vs CON or S). Thisprotection was partially reversed by administration of staurosporinein the 0.4MAC+S group (30[2]%; P<0.05 vs 0.4MAC) group, butnot after administration of 1 MAC or 1.75 MAC isoflurane (26[2]%and 31[2]%, respectively). Thus 0.4MAC increased PKC ${varepsilon}$ phosphorylation,and this effect was blocked by staurosporine. Higher concentrationsof isoflurane did not change PKC ${varepsilon}$ phosphorylation. PKC ${varepsilon}$ was translocatedto the membrane fraction after administration of 0.4 MAC isoflurane,but not after 1.0 or 1.75 MAC.

Conclusions. Although isoflurane preconditioning resulted ina reduction in infarct size at all concentrations used, theprotection was mediated by phosphorylation and translocationof PKC ${varepsilon}$ only at 0.4 MAC.

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British Journal of Anaesthesia

Role of protein kinase C- (PKC) in isoflurane-induced cardioprotection

Role of protein kinase C- ${varepsilon}$ (PKC ${varepsilon}$ ) in isoflurane-induced cardioprotection